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External regulation of immune response

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External regulation of immune response J. Ochotn Causal treatment a) Stem cell transplantation for serious congenital disorders of the immune system and some ... – PowerPoint PPT presentation

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Title: External regulation of immune response


1
External regulation of immune response
J. Ochotná
2
Causal treatment
  • a) Stem cell transplantation    
  • for serious congenital disorders of the immune
    system and some lymphoproliferative and
    myeloproliferative disorders
  • complications infectious complications
                        Graft-versus-host
  • obtaining stem cells - collection from shovel hip
    bone                              - from
    umbilical cord blood                             
     - from peripheral blood after stimulation
    with GM-CSF

3
  • b) Gene therapy
  • with a suitable expression vector is introduced
    functional gene (to replace dysfunctional gen)
    into the lymphocytes or stem cells
  • used as a treatment for some cases of SCID

4
Substitution treatment
  • autologous stem cell transplantation
    followingchemotherapy and radiotherapy
  • treatment with intravenous immunoglobulin
    (derived from plasma of blood donors)
  • substitution of C1 inhibitor for hereditary
    angioedema
  • substitution of erythropoietin in patients with
    chronic renal failure
  • substitution of G-CSF in agranulocytosis

5
Immunomodulation
  • medical procedure to adjust the disrupted
    immune function
  • Non-specific immunosuppressive therapy
  • nonspecific affects not only autoreactive and
    aloreactive                        lymphocytes,
    but also other components of
    immunity (risk of
    reduction antiinfectious and anti-
    tumor immunity)
  • used for treatment of autoimmune diseases, severe
    allergic conditions and for organ
    transplantation

6
Non-specific immunosuppressive therapy
  • corticosteroids - anti-inflammatory,
    immunosuppressive
    effects                    - blocking the
    activity of transcription
    factors (AP-1, NFkB)                   
    - suppress the expression of genes (IL-2,
    IL-1, phospholipase A, MHC
    gp II, adhesion
    molecules)                   - inhibition
    of histamine release from basophils
                       - higher concentrations
    induce apoptosis of
    lymfocytes
  • immunosuppressants affecting the metabolism of
    DNA - cyclophosphamide                       
       - methotrexate -
    azathioprine

7
  • immunosuppressant selectively inhibiting T
    lymphocytes - immunosuppressive ATB
    cyclosporine A, tacrolimus,
    rapamycin (suppressing the expression of IL-2 and
    IL-2R in activated T
    lymphocytes)                 - monoclonal
    antibody anti-CD3 (Immunosuppression
    after transplantation, treatment of
    rejection crises)
  • immunoglobulins in the immunosuppressive
    indication                  - Polyspecific
    intravenous immunoglobulins                    (I
    nhibition of B lymphocytes, antiidiotype
    activity, inhibition of
    cytokines, neutralization of toxins,
    inhibition of complement activation ...)

8
Anti-inflammatory and antiallergic treatment
  • nonsteroidal anti-inflammatory drugs
  • antihistamines - blocking H1 receptor
                             - reduce the expression
    of adhesion molecules
                             - reduce the secretion
    of histamine ...
  • inhibitors of inflammatory cytokine -
    receptor antagonist for IL-1                     
         - monoclonal antibodies against TNF
                             - thalidomide (TNF
    inhibitor)
  • enzyme therapy - in the enzyme mixture has a
    major effect
    trypsin and bromelain                           
    - anti-inflammatory
    and immunomodulatory effects

9
Non-specific immunostimulant therapy
  • synthetic immunomodulators
  • Methisoprinol (Isoprinosine) - used in viral
    infections with more
    severe or relapsing course
  • bacterial extracts and lysates
  • Broncho-Vaxom - prevention of recurrent
    respiratory tract infections
  • Ribomunyl
  • products of the immune system
  • IL-2 - renal adenocarcinoma
  • IFNa, IFNb - viral hepatitis, some leukemia
  • Erythropoietin renal failure
  • G-CSF, GM-CSF neutropenia
  • Transfer factor (blood donors leukocytes
    undergoing dialysis)
  • Thymus hormones              

10
Antigen-specific immunomodulatory therapy
  • specific immunomodulation induce an immune
    response or tolerance against a specific antigen
    a) active immunization use of antigen to
    induce an immune response that can later protect
    against a pathogen bearing the antigen (or
    similar antigen)
  • immunization vaccines are made from inactivated
    or attenuated microorganisms or their antigens
    (polysaccharide capsule, toxins)
  • creates long-term immunity
  • activate cellular and antibody immunity
  • administration of antigen injectable, oral
  • prophylaxis
  • risk of infection or anaphylactic reactions

11
  • b) passive immunization
  • natural - transfer of maternal antibodies in
    fetal blood
  • therapeutically - the use of animal antibodies
    against various
    toxins (snake toxins, tetanus
    toxin, botulinum toxin)
  • prophylaxis - the human immunoglobulin from
    immunized individuals (hepatitis
    A, rabies, tetanus)
                        - Anti-RhD antibodies -
    preventing maternal
    immunization with RhD fetus
  • provides a temporary (3 weeks) specific humoral
    immunity
  • the risk anaphylactic reactions

12
  • c) specific immunosuppression induction of
    tolerance against a specific antigen
  • ongoing clinical studies
  • induction of tolerance by oral administration of
    antigen (treatment of certain autoimmune
    diseases)
  • allergen immunotherapy (pollen, insect poisons)
  • d) vaccination against cancer
  • immunization by dendritic cells

13
Defence against extracellular pathogens
14
Defence against extracellular pathogens
  • bacteria (gram-negative, gram-positive cocci,
    bacilli), unicellular parasites
  • for their elimination is necessary opsonization
    (C3b, lectins, antibodies ...)
  • neutrophilic granulocytes are chemotactic
    attracting to the site of the infection (C5a, C3a
    and chemotactic products of bacteria)
  • absorbed bacteria are destroyed by the
    microbicidal systems (products of NADP-H
    oxidase, hydrolytic enzymes and bactericidal
    substances in lysosomes)

15
  • phagocytes produce proinflammatory cytokines
    (IL-1, IL-6, TNF) that induce an increase in
    temperature, metabolic response of the organism
    and synthesis of acute phase proteins
  • in later stages of infection are stimulated
    antigen-specific mechanisms
  • plasma cells initially produce IgM isotype after
    isotype switching produce IgG1 and IgA
    (opsonization)
  • sIgA protect against intestinal and respiratory
    infections by bacteria
  • bacteria with a polysaccharide capsule may cause
    T-independent IgM antibody production (after the
    establishment to the bacteria activate the
    classical complement path)

16
  • after infection persist IgG, IgA (protective
    effect) and memory T and B lymphocytes
  • in the defense against bacterial toxins apply
    neutralizing antibodies (Clostridium tetani and
    botulinum ...)
  • "indirect toxins - bacterial Lipopolysaccharide
    (LPS) stimulates big number of monocytes to
    release TNF, which can cause septic shock
  • extracellular bacterial infections are especially
    at risk individuals with disorders in the
    function of phagocytes, complement and antibody
    production

17
Defence against intracellular pathogens
18
Defense against intracellular pathogens
  • bacteria, fungi and unicellular parasites
  • intracellular parasites are resistant to the
    microbicidal mechanisms of phagocytes
  • macrophages, which absorbed them, produce IL-12 ?
    TH1 differentiation, production of IFNg and
    membrane TNF ? activation of macrophages and
    induction of iNOS
  • plasma cells under the influence of IFNg produce
    IgG2, immune complexes containing IgG2 bind to
    Fc receptors on macrophages and thus stimulate
    them-

19
  • in the defense against intracelular parasites,
    which escape from phagolysosomes apply TC
    lymphocytes
  • intracellular microorganisms infections are at
    risk individuals with certain disorders of
    phagocytes and defects of T lymphocytes

20
Defense against intracellular pathogens
21
Anti-viral defence
22
Anti-viral defence
  • interferons - in infected cells is induced
    production of IFNa and IFNb (prevents viral
    replication and in uninfected cells cause the
    anti-virus status) IFNg stimulates the
    conversion to activated macrophages (iNOS)
  • NK cells - ADCC (Antibody-dependent cell-mediated
    cytotoxicity) cytotoxic reaction depends on the
    antibodies the NK-lymphocyte recognizes cell
    opsonized with IgG by stimulation Fc receptor
    CD16 and then activate cytotoxic mechanisms
    (degranulation)
  • infected macrophages produce IL-12 (a strong
    activator of NK cells)

23
  • in the defense against cytopathic viruses mostly
    applied antibodies
  • sIgA inhibit mucosal adhesion of viruses (defense
    against respiratory viruses and enteroviruses)
  • neutralizing IgG and IgM antibodies activate the
    classical way of complement, which is capable of
    some viruses lysis
  • IgA and IgG derived in viral infection have a
    preventive effect in secondary infection

24
  • effector TC lymphocytes destroy infected cells in
    direct contact (granzym/perforin FasL) and by
    produced cytokines (lymfotoxin)
  • some viruses after infection integrate into the
    host genome, where persist for years (varicella
    zoster, EBV, papillomavirus)
  • by these infections are at risk individuals with
    T lymphocyte immunodeficiency and with combined
    immune disorders
  • increased susceptibility to herpes infections in
    individuals with dysfunction of NK cells

25
Defense against multicellular parasites
26
Defense against multicellular parasites
  • contact of mast cells, basophils and eosinophils
    with parasite antigens
  • TH2 stimulation under the influence of IL-4 (mast
    cells and other APC stimulated by parasite)
  • TH2 stimulate B cells with BCR-specific parasite
    antigens
  • isotype switching under the influence of IL-4 to
    IgE
  • IgE bind to FceRI on mast cells and basophils
    (antigen-specific receptors)

27
  • establish of multivalent antigen (multicellular
    parasite) using the IgE to highafinity Fc
    receptor for IgE (Fc?RI) aggregation of several
    molecules Fc?RI
  • initiate mast cell degranulation (cytoplasmic
    granules mergers with the surface membrane and
    release their contents)
  • activation of arachidonic acid metabolism
    (leukotriene C4, prostaglandin PGD2) -
    amplification of inflammatory responses
  • cytokine production by mast cell (TNF, TGF?,
    IL-4, 5,6 ...)

28
  • in later stages are activated TH1 and are
    produced antibodies of other classes
  • eosinophils fagocyte complexes of parasitic
    particles with IgE via their receptors for IgE
  • eosinophils use against parasites extracellular
    bactericidal substances released from granules
    (eosinophil cationic protein, protease)

29
Activation of mast cell
30
Anti-tumour immunology
31
  • Malignant transformation
  • failure of regulation of cell division and
    regulation of "social" behavior of the cells
  • the uncontrollable proliferation, dissemination
    to other tissues
  • mutations in protoonkogenes and antionkogenes
  • Tumor cells
  • unlimited growth
  • growth without stimulating growth factors
  • immortality
  • often altered number of chromosomes as frequent
    chromosomal alteration
  • TSA ...

32
Tumor antigens
  • Antigens specific for tumors (TSA)
  • complexes of MHCgp I with abnormal fragments of
    cellular proteins - chemically induced tumors
    - leukemia with
    chromosomal translocation
  • complexes of MHC gp with fragments of proteins of
    oncogenic viruses - tumors caused by viruses
    (EBV, SV40,
    polyomavirus)
  • abnormal forms of glycoproteins - sialylation of
    tumor cells
    surface proteins
  • idiotypes of myeloma and lymphoma - clonotyping
    TCR
    and BCR

33
  • b) Antigens associated with tumors (TAA)
  • present also on normal cells
  • differences in quantity, time and local
    expression
  • auxiliary diagnostic markers
  • 1) onkofetal antigens
  • on normal embryonic cells and some tumor cells
  • ?-fetoprotein (AFP) - hepatom
  • carcinoembryonic antigen (CEA) - colon cancer
  • 2) melanoma antigens
  • MAGE-1, Melan-A

34
  • 3) antigen HER2/neu
  • receptor for epithelial growth factor
  • mammary carcinoma
  • 4) EPCAM
  • epithelial adhesion molecule
  • metastases
  • 5) differentiation antigens of leukemic cells
  • present on normal cells of leukocytes linage
  • CALLA -acute lymphoblastic leukemia (CD10 pre-B
    cells)

35
Anti-tumor immune mechanisms
  • Immune control
  • tumor cells normally arise in tissues
  • and are eliminated by T lymphocytes
  • probably wrong hypothesis
  • Defensive immune response
  • tumor cells are weakly immunogenic
  • occurs when tumor antigens are presented to T
    lymphocytes by dendritic cells activated in the
    inflammatory environment
  • if tumor cells are detected, in defense may be
    involved non-specific mechanisms (neutrophilic
    granulocytes, macrophages, NK cells) and
    antigen-specific mechanisms (complement
    activating antibodies or ADCC, TH1 and TC)

36
  • cancer-associated antigens are processed by APC
    and recognized by T lymphocytes in complex with
    HLA I. and II. class with providing costimulus
    signals
  • predominance of TH1 (IFN g, TNFa)
  • specific cell-mediated cytotoxic reactivity TC
  • activation of TH2 ? support B lymphocytes? tumor
    specific antibodies (involved in the ADCC)
  • tumor cells are destroyed by cytotoxic NK cells
    (ADCC)

37
Anti-tumor immune mechanisms
38
Mechanisms of tumor resistance to the immune
system
  • -
  • high variability of tumor cells
  • low expression of tumor antigens
  • sialylation
  • tumor cells signals do not provide costimulus ? T
    lymphocyte anergy
  • some anticancer substances have a stimulating
    effect
  • production of factors inactivating T lymphocytes
  • expression of FasL ? T lymphocyte apoptosis
  • inhibition of the function or durability
    dendritic cells (NO, IL-10, TGF-b)

39
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